The distinct cognitive syndromes of Parkinson's disease: 5 year follow-up of the CamPaIGN cohort

doi:10.1093/brain/awp245

Brain Advance Access originally published online on October 7, 2009
Brain 2009 132(11):2958-2969; doi:10.1093/brain/awp245

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The distinct cognitive syndromes of Parkinson's disease: 5 year follow-up of the CamPaIGN cohort

Caroline H. Williams-Gray¹, Jonathan R. Evans¹, An Goris²^,3, Thomas Foltynie⁴, Maria Ban², Trevor W. Robbins⁵, Carol Brayne⁶, Bhaskar S. Kolachana⁷, Daniel R. Weinberger⁷, Stephen J. Sawcer² and Roger A. Barker¹

1 Centre for Brain Repair, Department of Clinical Neurosciences, University of Cambridge, UK 2 Neurology Unit, Department of Clinical Neurosciences, University of Cambridge, UK 3 Laboratory for Neuroimmunology, Section for Experimental Neurology, Katholieke Universiteit Leuven, Leuven, Belgium 4 Sobell Department of Motor Neuroscience and Movement Disorders, Institute of Neurology, University College London, UK 5 Department of Experimental Psychology, University of Cambridge, UK 6 Department of Public Health and Primary Care, University of Cambridge, UK 7 Genes, Cognition and Psychosis Program, National Institute of Mental Health Intramural Research Program, National Institutes of Health, Department of Health and Human Services, Bethesda, MD, USA

Correspondence to: Caroline H. Williams-Gray, Cambridge Centre for Brain Repair, Department of Clinical Neurosciences, University of Cambridge, Forvie Site, Robinson Way, Cambridge, CB2 0PY, UK E-mail: chm27{at}cam.ac.uk

Cognitive abnormalities are common in Parkinson's disease, withimportant social and economic implications. Factors influencingtheir evolution remain unclear but are crucial to the developmentof targeted therapeutic strategies. We have investigated thedevelopment of cognitive impairment and dementia in Parkinson'sdisease using a longitudinal approach in a population-representativeincident cohort (CamPaIGN study, n = 126) and here present the5-year follow-up data from this study. Our previous work hasimplicated two genetic factors in the development of cognitivedysfunction in Parkinson's disease, namely the genes for catechol-O-methyltransferase(COMT Val¹⁵⁸Met) and microtubule-associated protein tau (MAPT)H1/H2. Here, we have explored the influence of these genes inour incident cohort and an additional cross-sectional prevalentcohort (n = 386), and investigated the effect of MAPT H1/H2haplotypes on tau transcription in post-mortem brain samplesfrom patients with Lewy body disease and controls. Seventeenpercent of incident patients developed dementia over 5 years[incidence 38.7 (23.9–59.3) per 1000 person-years]. Wehave demonstrated that three baseline measures, namely, age $≥$ 72 years, semantic fluency less than 20 words in 90 s and inabilityto copy an intersecting pentagons figure, are significant predictorsof dementia risk, thus validating our previous findings. Incombination, these factors had an odds ratio of 88 for dementiawithin the first 5 years from diagnosis and may reflect thesyndrome of mild cognitive impairment of Parkinson's disease.Phonemic fluency and other frontally based tasks were not associatedwith dementia risk. MAPT H1/H1 genotype was an independent predictorof dementia risk (odds ratio = 12.1) and the H1 versus H2 haplotypewas associated with a 20% increase in transcription of 4-repeattau in Lewy body disease brains. In contrast, COMT genotypehad no effect on dementia, but a significant impact on Towerof London performance, a frontostriatally based executive task,which was dynamic, such that the ability to solve this taskchanged with disease progression. Hence, we have identifiedthree highly informative predictors of dementia in Parkinson'sdisease, which can be easily translated into the clinic, andestablished that MAPT H1/H1 genotype is an important risk factorwith functional effects on tau transcription. Our work suggeststhat the dementing process in Parkinson's disease is predictableand related to tau while frontal-executive dysfunction evolvesindependently with a more dopaminergic basis and better prognosis.

Key Words: Parkinson's disease; dementia; cognitive deficits; microtubule-associated protein tau; catechol-O-methyltransferase

Abbreviations: COMT, the gene coding for catechol-O-methyltransferase; gDNA, genomic DNA; MAPT, the gene coding for microtubule-associated protein tau; MCI, mild cognitive impairment; OR, odds ratio; PIGD, postural instability and gait disturbance; PRM, Pattern Recognition Memory; SRM, Spatial Recognition Memory; TOL, Tower of London

Received May 20, 2009. Revised July 23, 2009. Accepted August 19, 2009.

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